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14 results on '"Delpe-Acharige A"'

1. Pyrazolyl Thioureas and Carbothioamides with an NNSN Motif against MSSA and MRSA

Author

Anjana Delpe-Acharige, Man Zhang, Kayla Eschliman, Alex Dalecki, Obdulia Covarrubias-Zambrano, Azriel Minjarez-Almeida, Tejaswi Shrestha, Tanji Lewis, Fatimah Al-Ibrahim, Sophia Leonard, Riana Roberts, Anteneh Tebeje, Aruni P. Malalasekera, Hongwang Wang, Madumali Kalubowilage, Frank Wolschendorf, Olaf Kutsch, and Stefan H. Bossmann

Subjects
Chemistry, QD1-999
Published
2021
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2. Pyrazolyl Thioureas and Carbothioamides with an NNSN Motif against MSSA and MRSA

Author

Alex G. Dalecki, Obdulia Covarrubias-Zambrano, Riana Roberts, Frank Wolschendorf, Tanji Lewis, Tejaswi Shrestha, Fatimah Al-Ibrahim, Stefan H. Bossmann, Hongwang Wang, Sophia Leonard, Aruni P. Malalasekera, Olaf Kutsch, Madumali Kalubowilage, Kayla Eschliman, Azriel Minjarez-Almeida, Man Zhang, Anteneh Tebeje, and Anjana Delpe-Acharige

Subjects
Drug, Strain (chemistry), Chemistry, General Chemical Engineering, media_common.quotation_subject, General Chemistry, biochemical phenomena, metabolism, and nutrition, medicine.disease_cause, bacterial infections and mycoses, Article, Microbiology, Staphylococcus aureus, medicine, bacteria, Structural motif, QD1-999, media_common
Abstract

A novel series of copper-activatable drugs intended for use against methicillin-sensitive Staphylococcus aureus (MSSA) and methicillin-resistant S. aureus (MRSA) were synthesized, characterized, and tested against the MSSA strain Newman and the MRSA Lac strain (a USA300 strain), respectively. These drugs feature an NNSN structural motif, which enables the binding of copper. In the absence of copper, no activity against MSSA and MRSA at realistic drug concentrations was observed. Although none of the novel drug candidates exhibits a stereocenter, sub-micromolar activities against SA Newman and micromolar activities against SA Lac were observed in the presence, but not in the absence, of bioavailable copper. Copper influx is a component of cellular response to bacterial infections, which is often described as nutritional immunity.

Published
2021

3. A Catalyst-Free, Temperature-Driven One-Pot Synthesis of 1-Adamantylhydrazine Hydrochloride

Author

James Hodgson, Stefan H. Bossmann, Anjana M. D. S. Delpe Acharige, and Raul Neri

Subjects
0303 health sciences, 010405 organic chemistry, 030306 microbiology, Hydrochloride, Organic Chemistry, Extraction (chemistry), One-pot synthesis, Organic layer, 01 natural sciences, Combinatorial chemistry, Catalysis, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, chemistry, Yield (chemistry), Extraction methods
Abstract

1-Adamantylhydrazine can be a versatile intermediate for many biologically active compounds as adamantyl possesses a wide spectrum of medicinal properties. Described here is a detailed one-pot synthesis of 1-adamantylhydrazine, carried out on a milligram to gram scale, that steadily delivers a highly stable product used to carry out the synthesis of 1-(adamantan-1-yl)-1H-pyrazol-3-amine for bacterial studies. The reaction employs inexpensive, catalyst free, readily available starting materials. In the synthesis of 1-(adamantan-1-yl)-1H-pyrazol-3-amine, the use of a continuous extraction method allows for complete extraction of the target product into the organic layer and increases the overall percentage yield.

Published
2020
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4. Practical and scalable synthesis of beclomethasone dipropionate

Author

Dhanushi T. Welideniya, Adeesha S. Jayathilaka, Anjana Delpe Acharige, K.A.U. Samanthi, Umayangani K. Wanninayake, Shashika S. Perera, Weranga Rajapaksha, Chamod C. Fernando, Madhavi Hewadikaram, Janani Buddhika, Pivini Gunasekara, Veranja Karunaratne, G.A.J. Amaratunga, and Dinara S. Gunasekera

Subjects
Pharmacology, Endocrinology, Organic Chemistry, Clinical Biochemistry, Beclomethasone, Molecular Conformation, Stereoisomerism, Molecular Biology, Biochemistry
Abstract

Beclomethasone dipropionate (1) is a synthetic corticosteroid with anti-inflammatory, antipruritic, and anti-allergy properties. It is widely used to treat asthma, allergic rhinitis, and dermatoses. However, existing synthetic routes to this active pharmaceutical ingredient (API) contain steps resulting in low and/or inconsistent yields, and use obsolete reagents. Such inconsistencies coupled with a lack of reliable experimental data makes laboratory-scale and large-scale synthesis of this API difficult and time-consuming. In this paper, we report a practical and scalable approach to synthesize 1 from the readily available steroidal intermediate, 16β-methyl epoxide (3, DB-11). A gram-scale to kilogram-scale synthesis of 1 was achieved with 82% yield, using a cost-effective and scalable methodology. Selective propionylation of the hydroxyl groups at C

Published
2021

5. Updating Levothyroxine Synthesis for the Modern Age

Author

Anjana Delpe Acharige, Veranja Karunaratne, Dinara S. Gunasekera, Gehan A. J. Amaratunga, Adeesha Saseenda Jayathilaka, Shashika Sevvandi Perera, Umayangani K. Wanninayake, Upamalika Samanthi, Dhanushi Welideniya, and Shihan Shalinda Kaleel

Subjects
Active ingredient, business.industry, Chemistry, Organic Chemistry, Levothyroxine, medicine, Fine chemical, Process engineering, business, Biochemistry, Levothyroxine Sodium, medicine.drug, Sodium salt
Abstract

Synthesis of levothyroxine sodium, the sodium salt of a synthetic levoisomer of thyroxine, revolutionized the management of hypothyroidism and related symptoms. However, the primary synthetic route to this active pharmaceutical ingredient (API) is more than 70+ years old with low-yielding steps and obsolete reagents. It lacks experimental data on intermediates, making laboratory and large-scale synthesis of this API difficult and time-consuming. Here, we describe an improved synthesis of levothyroxine using commonly available modern reagents. By modifying and replacing low yielding and/or unproductive steps of Chalmers synthesis, we were able to achieve higher overall yields (39-51%) consistently. Key modifications include an alternative path to the selective N-acetylation step that yielded 5 in a pure and consistent fashion. Our improved methodology, coupled with detailed experimental data, provides a practical alternative to existing methods that can be conveniently implemented to synthesize Levothyroxine sodium in fine chemical settings.

Published
2020

6. An efficient and high-yielding method for extraction and purification of linamarin from Cassava;

Author

K A U, Samanthi, Dhanushi T, Welideniya, Anjana Delpe, Acharige, Sameera R, Samarakoon, Rajitha K, Rathnayaka, Madhavi, de Silva, Shashika S, Perera, Colin, Pieris, Umayangani K, Wanninayake, Adeesha, Jayathilaka, Veranja, Karunaratne, G A J, Amaratunga, and Dinara S, Gunasekera

Subjects
Manihot, Nitriles, Vegetables
Abstract

During the last three decades, studies of linamarin extracted from cassava have received increased attention due to the presence of high cyanogenic compounds in these extracts. The methods that are utilized to isolate linamarin are either tedious or use acidic conditions resulting in poor yields. In this study, a novel cryocooled method of extraction has been developed to isolate linamarin from Cassava root peel. Approximately 18 g of linamarin was isolated from 1 kg of fresh Cassava root peel, which is the highest amount reported to date. Linamarin was fully characterized using NMR, IR and LCMS. The anti-cancer properties of pure linamarin and Cassava crude extract were evaluated by a comprehensive cytotoxic assay, using MCF-7, HepG2, NCI H-292, AN3CA and MRC-5 cell lines. The crude extract showed higher cytotoxicity compared to pure linamarin. The results of the biological evaluation are comparable to other reported studies in the literature.

Published
2020

7. An efficient and high-yielding method for extraction and purification of linamarin from Cassava; in vitro biological evaluation

Author

K.A.U. Samanthi, Madhavi de Silva, Adeesha Saseenda Jayathilaka, Shashika Sevvandi Perera, Veranja Karunaratne, Rajitha K Rathnayaka, Dhanushi Welideniya, Colin Pieris, Gehan A. J. Amaratunga, Sameera R. Samarakoon, Anjana Delpe Acharige, Umayangani K. Wanninayake, and Dinara S. Gunasekera

Subjects
Chromatography, Chemistry, Organic Chemistry, Extraction (chemistry), food and beverages, Plant Science, Linamarin, Biochemistry, High yielding, In vitro, Analytical Chemistry, chemistry.chemical_compound, Cytotoxicity, Biological evaluation
Abstract

During the last three decades, studies of linamarin extracted from cassava have received increased attention due to the presence of high cyanogenic compounds in these extracts. The methods that are utilized to isolate linamarin are either tedious or use acidic conditions resulting in poor yields. In this study, a novel cryocooled method of extraction has been developed to isolate linamarin from Cassava root peel. Approximately 18 g of linamarin was isolated from 1 kg of fresh Cassava root peel, which is the highest amount reported to date. Linamarin was fully characterized using NMR, IR and LCMS. The anti-cancer properties of pure linamarin and Cassava crude extract were evaluated by a comprehensive cytotoxic assay, using MCF-7, HepG2, NCI H-292, AN3CA and MRC-5 cell lines. The crude extract showed higher cytotoxicity compared to pure linamarin. The results of the biological evaluation are comparable to other reported studies in the literature.

Published
2020
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8. Pyrazolyl Thioureas and Carbothioamides with an NNSN Motif against MSSA and MRSA

Author

Delpe-Acharige, Anjana, primary, Zhang, Man, additional, Eschliman, Kayla, additional, Dalecki, Alex, additional, Covarrubias-Zambrano, Obdulia, additional, Minjarez-Almeida, Azriel, additional, Shrestha, Tejaswi, additional, Lewis, Tanji, additional, Al-Ibrahim, Fatimah, additional, Leonard, Sophia, additional, Roberts, Riana, additional, Tebeje, Anteneh, additional, Malalasekera, Aruni P., additional, Wang, Hongwang, additional, Kalubowilage, Madumali, additional, Wolschendorf, Frank, additional, Kutsch, Olaf, additional, and Bossmann, Stefan H., additional

Published
2021
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10. Computational insights into the inhibition of β-haematin crystallization by antimalarial drugs

Author

Marcus C. Durrant, Kate Lauder, Anjana M. D. S. Delpe Acharige, Mark P. C. Brennan, Adesola O. Odebunmi, and Fiona McMahon

Subjects
Models, Molecular, Drug, Iron, media_common.quotation_subject, Molecular Conformation, Protoporphyrins, B200, 010402 general chemistry, 01 natural sciences, Haematin, law.invention, Inorganic Chemistry, Antimalarials, chemistry.chemical_compound, Deprotonation, law, Monolayer, Molecule, Crystallization, Mode of action, media_common, 010405 organic chemistry, Combinatorial chemistry, 0104 chemical sciences, chemistry, Hemin, Density functional theory
Abstract

During the red blood cell phase of their life cycle, malaria parasites digest their host's haemoglobin, with concomitant release of potentially toxic iron(iii) protoporphyrin IX (FePPIX). The parasites' strategy for detoxification of FePPIX involves its crystallization to haemozoin, such that the build-up of free haem in solution is avoided. Antimalarial drugs of both historical importance and current clinical use are known to be capable of disrupting the growth of crystals of β-haematin, which is the synthetic equivalent of haemozoin. Hence, the disruption of haemozoin crystal growth is implicated as a possible mode of action of such drugs. However, the details of β-haematin crystal poisoning at the molecular level have yet to be fully elucidated. In this study, we have used a combination of density functional theory (DFT) and molecular modelling to examine the possible modes of action of ten different antimalarial drugs, including quinine-type aliphatic alcohols, amodiaquine-type phenols, and chloroquine-type aliphatic diamines. The DFT calculations indicate that each of the drugs can form at least one molecular complex with FePPIX. These complexes have 1 : 1 or 2 : 1 FePPIX : drug stoichiometries and all of them incorporate Fe-O bonds, formed either by direct coordination of a zwitterionic form of the drug, or by deprotonation of water. Most of the drugs can form more than one such complex. We have used the DFT model structures to explore the possible formation of a monolayer of each drug-haem complex on four of the β-haematin crystal faces. In all cases, the drug complexes can form a monolayer on the fast-growing {001} and {011} faces, but not on the slower growing {010} and {100} faces. Additional modelling of the chloroquine and quinidine complexes shows that individual molecules of these species can also obstruct the growth of new layers on other crystal faces. The implications of these observations for antimalarial drug development are discussed.

Published
2018

11. A Catalyst-Free, Temperature-Driven One-Pot Synthesis of 1-Adamantylhydrazine Hydrochloride.

Author

Delpe Acharige, Anjana, Neri, Raul, Hodgson, James, and Bossmann, Stefan H.

Subjects
*BIOACTIVE compounds, *ORGANIC products, *CATALYSTS
Abstract

1-Adamantylhydrazine can be a versatile intermediate for many biologically active compounds as adamantyl possesses a wide spectrum of medicinal properties. Described here is a detailed one-pot synthesis of 1-adamantylhydrazine, carried out on a milligram to gram scale, that steadily delivers a highly stable product used to carry out the synthesis of 1-(adamantan-1-yl)-1 H -pyrazol-3-amine for bacterial studies. The reaction employs inexpensive, catalyst free, readily available starting materials. In the synthesis of 1-(adamantan-1-yl)-1 H -pyrazol-3-amine, the use of a continuous extraction method allows for complete extraction of the target product into the organic layer and increases the overall percentage yield. [ABSTRACT FROM AUTHOR]

Published
2020
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13. An atomic scale mechanism for the antimalarial action of chloroquine from density functional theory calculations

Author

Marcus C. Durrant and Anjana M. D. S. Delpe Acharige

Subjects
Metals and Alloys, Crystal structure, C700, Atomic units, Inorganic Chemistry, Solvent, chemistry.chemical_compound, chemistry, Halofantrine, Computational chemistry, Atom, Alkoxide, Materials Chemistry, Density functional theory, Organometallic chemistry
Abstract

The X-ray crystal structures of complexes between the antimalarial drugs quinine, quinidine and halofantrine and their biological target, iron(III) ferriprotoporphyrin IX (FePPIX), have been reported in the literature (de Villiers et al. in ACS Chem Biol 7:666, 2012; J Inorg Biochem 102:1660, 2008) and show that all three drugs utilize their zwitterionic alkoxide forms to coordinate to the iron atom via Fe–O bonds. In this work, density functional theory calculations with implicit solvent corrections have been used to model the energetics of formation of these complexes. It is found that the cost of formation of the active zwitterionic form of each drug is more than offset by the energy of its binding to FePPIX, such that the overall energies for complexation of all three drugs with FePPIX are moderately favourable in water, and rather more favourable in n-octanol as solvent. The calculations have been extended to develop an analogous model for the complex between FePPIX and chloroquine, whose structure is not presently known from experiment.

Published
2014

14. Antioxidant, anti-tyrosinase, hepatoprotective, and anti-inflammatory potential in flowers and seeds of Ochna integerrima (Lour.) Merr.

Author

Minh Nguyen H, Nguyen KP, Le ATP, Nguyen NHT, Vu-Huynh LK, Le CKT, Delpe Acharige A, Hull K, and Romo D

Abstract

This study explored, for the first time, the antioxidant (total antioxidant content, reducing power, ferric ion reducing antioxidant power, hydroxyl radical scavenging, ferrous ion-chelating assays), anti-tyrosinase, anti-inflammatory properties, and hepatoprotective effect in HepG2 cell lines of Ochna integerrima (Loureiro) Merrill flowers and seeds. All extracts except n -hexane exhibited significant antioxidant activity, with high levels of tannin and proanthocyanidins. Luteolin ( 1 ), 6- γ , γ -dimethylallylkaempferol7- O - β -d-glucopyranoside ( 2 ), 6- γ , γ -dimethylallylquercetin7- O - β -d-glucopyranoside ( 3 ), and 6- γ , γ -dimethylallyldihydrokaempferol 7- O - β -d-glucopyranoside ( 4 ) were isolated using semi-preparative HPLC. Compounds 1 - 3 demonstrated good anti-tyrosinase activity. The most active hepatoprotective extracts were found to be aqueous extracts. The flower extracts exhibited greater anti-inflammatory properties by the decrease of NO in RAW 264.7 cells and bovine serum albumin protein. Among them, the n -hexane and EtOAc extracts from flowers displayed promising anti-inflammatory activity. This was predicted by in silico analysis of 1 - 4 . In summary, O. integerrima appears to be a promising natural source for antioxidant, anti-tyrosinase, and anti-inflammatory applications.

Published
2024
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